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1. Datopotamab–deruxtecan plus durvalumab in early-stage breast cancer: the sequential multiple assignment randomized I-SPY2.2 phase 2 trial

Author

Shatsky, Rebecca A, Trivedi, Meghna S, Yau, Christina, Nanda, Rita, Rugo, Hope S, Davidian, Marie, Tsiatis, Butch, Wallace, Anne M, Chien, A Jo, Stringer-Reasor, Erica, Boughey, Judy C, Omene, Coral, Rozenblit, Mariya, Kalinsky, Kevin, Elias, Anthony D, Vaklavas, Christos, Beckwith, Heather, Williams, Nicole, Arora, Mili, Nangia, Chaitali, Roussos Torres, Evanthia T, Thomas, Brittani, Albain, Kathy S, Clark, Amy S, Falkson, Carla, Hershman, Dawn L, Isaacs, Claudine, Thomas, Alexandra, Tseng, Jennifer, Sanford, Amy, Yeung, Kay, Boles, Sarah, Chen, Yunni Yi, Huppert, Laura, Jahan, Nusrat, Parker, Catherine, Giridhar, Karthik, Howard, Frederick M, Blackwood, M Michele, Sanft, Tara, Li, Wen, Onishi, Natsuko, Asare, Adam L, Beineke, Philip, Norwood, Peter, Brown-Swigart, Lamorna, Hirst, Gillian L, Matthews, Jeffrey B, Moore, Brian, Symmans, W Fraser, Price, Elissa, Heditsian, Diane, LeStage, Barbara, Perlmutter, Jane, Pohlmann, Paula, DeMichele, Angela, Yee, Douglas, van ’t Veer, Laura J, Hylton, Nola M, and Esserman, Laura J

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Clinical Trials and Supportive Activities, Precision Medicine, Women's Health, Cancer, Clinical Research, Breast Cancer, 6.1 Pharmaceuticals, Good Health and Well Being, Medical and Health Sciences, Immunology, Biomedical and clinical sciences, Health sciences
Abstract

Sequential adaptive trial designs can help accomplish the goals of personalized medicine, optimizing outcomes and avoiding unnecessary toxicity. Here we describe the results of incorporating a promising antibody-drug conjugate, datopotamab-deruxtecan (Dato-DXd) in combination with programmed cell death-ligand 1 inhibitor, durvalumab, as the first sequence of therapy in the I-SPY2.2 phase 2 neoadjuvant sequential multiple assignment randomization trial for high-risk stage 2/3 breast cancer. The trial includes three blocks of treatment, with initial randomization to different experimental agent(s) (block A), followed by a taxane-based regimen tailored to tumor subtype (block B), followed by doxorubicin-cyclophosphamide (block C). Subtype-specific algorithms based on magnetic resonance imaging volume change and core biopsy guide treatment redirection after each block, including the option of early surgical resection in patients predicted to have a high likelihood of pathologic complete response, which is the primary endpoint assessed when resection occurs. There are two primary efficacy analyses: after block A and across all blocks for six prespecified HER2-negative subtypes (defined by hormone receptor status and/or response-predictive subtypes). In total, 106 patients were treated with Dato-DXd/durvalumab in block A. In the immune-positive subtype, Dato-DXd/durvalumab exceeded the prespecified threshold for success (graduated) after block A; and across all blocks, pathologic complete response rates were equivalent to the rate expected for the standard of care (79%), but 54% achieved that result after Dato-DXd/durvalumab alone (block A) and 92% without doxorubicin-cyclophosphamide (after blocks A + B). The treatment strategy across all blocks graduated in the hormone-negative/immune-negative subtype. No new toxicities were observed. Stomatitis was the most common side effect in block A. No patients receiving block A treatment alone had adrenal insufficiency. Dato-DXd/durvalumab is a promising therapy combination that can eliminate standard chemotherapy in many patients, particularly the immune-positive subtype.ClinicalTrials.gov registration: NCT01042379 .

Published
2024

3. Discovery and validation of a novel subgroup and therapeutic target in idiopathic multicentric Castleman disease

Author

Pierson, Sheila K., Shenoy, Sushila, Oromendia, Ana B., Gorzewski, Alexander M., Langan Pai, Ruth-Anne, Nabel, Christopher Shield, Ruth, Jason R., Parente, Sophia A.T., Arenas, Daniel J., Guilfoyle, Mary, Reddy, Manjula, Weinblatt, Michael, Shadick, Nancy, Bower, Mark, Pria, Alessia Dalla, Masaki, Yasufumi, Katz, Laura, Mezey, Jason, Beineke, Philip, Lee, David, Tendler, Craig, Kambayashi, Taku, Fosså, Alexander, van Rhee, Frits, and Fajgenbaum, David C.

Published
2021
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6. Multicenter Validation of the Diagnostic Accuracy of a Blood-Based Gene Expression Test for Assessing Obstructive Coronary Artery Disease in Nondiabetic Patients

Author

Rosenberg, Steven, Elashoff, Michael R., Beineke, Philip, Daniels, Susan E., Wingrove, James A., Tingley, Whittemore G., Sager, Philip T., Sehnert, Amy J., Yau, May, Kraus, William E., Newby, L. Kristin, Schwartz, Robert S., Voros, Szilard, Ellis, Stephen G., Tahirkheli, Naeem, Waksman, Ron, McPherson, John, Lansky, Alexandra, Winn, Mary E., Schork, Nicholas J., and Topol, Eric J.

Published
2010

7. A whole blood gene expression-based signature for smoking status

Author

Beineke Philip, Fitch Karen, Tao Heng, Elashoff Michael R, Rosenberg Steven, Kraus William E, and Wingrove James A

Subjects
Smoking, Gene expression, Coronary artery disease, Whole blood, Internal medicine, RC31-1245, Genetics, QH426-470
Abstract

Abstract Background Smoking is the leading cause of preventable death worldwide and has been shown to increase the risk of multiple diseases including coronary artery disease (CAD). We sought to identify genes whose levels of expression in whole blood correlate with self-reported smoking status. Methods Microarrays were used to identify gene expression changes in whole blood which correlated with self-reported smoking status; a set of significant genes from the microarray analysis were validated by qRT-PCR in an independent set of subjects. Stepwise forward logistic regression was performed using the qRT-PCR data to create a predictive model whose performance was validated in an independent set of subjects and compared to cotinine, a nicotine metabolite. Results Microarray analysis of whole blood RNA from 209 PREDICT subjects (41 current smokers, 4 quit ≤ 2 months, 64 quit > 2 months, 100 never smoked; NCT00500617) identified 4214 genes significantly correlated with self-reported smoking status. qRT-PCR was performed on 1,071 PREDICT subjects across 256 microarray genes significantly correlated with smoking or CAD. A five gene (CLDND1, LRRN3, MUC1, GOPC, LEF1) predictive model, derived from the qRT-PCR data using stepwise forward logistic regression, had a cross-validated mean AUC of 0.93 (sensitivity=0.78; specificity=0.95), and was validated using 180 independent PREDICT subjects (AUC=0.82, CI 0.69-0.94; sensitivity=0.63; specificity=0.94). Plasma from the 180 validation subjects was used to assess levels of cotinine; a model using a threshold of 10 ng/ml cotinine resulted in an AUC of 0.89 (CI 0.81-0.97; sensitivity=0.81; specificity=0.97; kappa with expression model = 0.53). Conclusion We have constructed and validated a whole blood gene expression score for the evaluation of smoking status, demonstrating that clinical and environmental factors contributing to cardiovascular disease risk can be assessed by gene expression.

Published
2012
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8. Quantitative Changes in Serum Proteins Including CXCL13 Are Early Indicators of Response to Anti-IL6 Therapy in Idiopathic Multicentric Castleman Disease

Author

Pierson, Sheila K, primary, Katz, Laura, additional, Nabel, Christopher Sheild, additional, Ruth, Jason R, additional, Diamond, Sheila, additional, Karvir, Hrishikesh, additional, Zhang, Fanyi, additional, Reddy, Manjula P, additional, Guilfoyle, Mary, additional, Tendler, Craig, additional, van Rhee, Frits, additional, Beineke, Philip, additional, Oromendia, Ana B, additional, and Fajgenbaum, David C, additional

Published
2019
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9. Development of a blood-based gene expression algorithm for assessment of obstructive coronary artery disease in non-diabetic patients

Author

Ellis Stephen G, Schwartz Robert S, Ginsburg Geoffrey S, Kraus William E, Voros Szilard, Rosenberg Steven, Tingley Whittemore G, Daniels Susan E, Beineke Philip, Wingrove James A, Elashoff Michael R, Tahirkheli Naheem, Waksman Ron, McPherson John, Lansky Alexandra J, and Topol Eric J

Subjects
Atherosclerosis, gene expression, whole blood classifier, Internal medicine, RC31-1245, Genetics, QH426-470
Abstract

Abstract Background Alterations in gene expression in peripheral blood cells have been shown to be sensitive to the presence and extent of coronary artery disease (CAD). A non-invasive blood test that could reliably assess obstructive CAD likelihood would have diagnostic utility. Results Microarray analysis of RNA samples from a 195 patient Duke CATHGEN registry case:control cohort yielded 2,438 genes with significant CAD association (p < 0.05), and identified the clinical/demographic factors with the largest effects on gene expression as age, sex, and diabetic status. RT-PCR analysis of 88 CAD classifier genes confirmed that diabetic status was the largest clinical factor affecting CAD associated gene expression changes. A second microarray cohort analysis limited to non-diabetics from the multi-center PREDICT study (198 patients; 99 case: control pairs matched for age and sex) evaluated gene expression, clinical, and cell population predictors of CAD and yielded 5,935 CAD genes (p < 0.05) with an intersection of 655 genes with the CATHGEN results. Biological pathway (gene ontology and literature) and statistical analyses (hierarchical clustering and logistic regression) were used in combination to select 113 genes for RT-PCR analysis including CAD classifiers, cell-type specific markers, and normalization genes. RT-PCR analysis of these 113 genes in a PREDICT cohort of 640 non-diabetic subject samples was used for algorithm development. Gene expression correlations identified clusters of CAD classifier genes which were reduced to meta-genes using LASSO. The final classifier for assessment of obstructive CAD was derived by Ridge Regression and contained sex-specific age functions and 6 meta-gene terms, comprising 23 genes. This algorithm showed a cross-validated estimated AUC = 0.77 (95% CI 0.73-0.81) in ROC analysis. Conclusions We have developed a whole blood classifier based on gene expression, age and sex for the assessment of obstructive CAD in non-diabetic patients from a combination of microarray and RT-PCR data derived from studies of patients clinically indicated for invasive angiography. Clinical trial registration information PREDICT, Personalized Risk Evaluation and Diagnosis in the Coronary Tree, http://www.clinicaltrials.gov, NCT00500617

Published
2011
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10. Serum Proteomics Reveals Distinct Subtypes Associated with Treatment Response in Idiopathic Multicentric Castleman Disease

Author

Shilling, Dustin, primary, Ruth, Jason R, additional, Nabel, Christopher Sheild, additional, Pierson, Sheila K, additional, Guilfoyle, Mary, additional, Tendler, Craig, additional, Reddy, Manjula P, additional, Weinblatt, Michael, additional, Shadick, Nancy, additional, Bower, Mark, additional, Dalla Pria, Alessia, additional, Masaki, Yasufumi, additional, Beineke, Philip, additional, Miljovska, Sofija, additional, Katz, Laura, additional, Shenoy, Sushila, additional, Oromendia, Ana B, additional, Mezey, Jason, additional, Wiser, Jeff, additional, Benbanaste, Jef, additional, Lee, David, additional, Fosså, Alexander, additional, van Rhee, Frits, additional, and Fajgenbaum, David C, additional

Published
2018
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13. IMPROVED DIAGNOSTIC WORK-UP OF PATIENTS PRESENTING TO THE CARDIOLOGIST WITH SYMPTOMS OF SUSPECTED OBSTRUCTS CORONARY ARTERY DISEASE: GENDER SPECIFIC RESULTS FROM THE IMPACT (INVESTIGATION OF A MOLECULAR PERSONALIZED CORONARY GENE EXPRESSION TEST ON CARDIOLOGY PRACTICE PATTERN) TRIAL

Author

McPherson, John A., primary, Davis, Kelly, additional, Yau, May, additional, Beineke, Philip, additional, Monane, Mark, additional, and Fredi, Joseph, additional

Published
2013
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15. Development of a blood-based gene expression algorithm for assessment of obstructive coronary artery disease in non-diabetic patients

Author

Elashoff, Michael R, primary, Wingrove, James A, additional, Beineke, Philip, additional, Daniels, Susan E, additional, Tingley, Whittemore G, additional, Rosenberg, Steven, additional, Voros, Szilard, additional, Kraus, William E, additional, Ginsburg, Geoffrey S, additional, Schwartz, Robert S, additional, Ellis, Stephen G, additional, Tahirkheli, Naheem, additional, Waksman, Ron, additional, McPherson, John, additional, Lansky, Alexandra J, additional, and Topol, Eric J, additional

Published
2011
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18. Evaluation of a solid matrix for collection and ambient storage of RNA from whole blood.

Author

Heng Tao, Beineke, Philip, Bing Li, Alberts, William, Rosenberg, Steven, Kvam, Erik, and Wingrove, James A.

Subjects
*EVALUATION, *RNA, *BLOOD, *MATRICES (Mathematics), *TEMPERATURE
Abstract

Background Whole blood gene expression-based molecular diagnostic tests are becoming increasingly available. Conventional tube-based methods for obtaining RNA from whole blood can be limited by phlebotomy, volume requirements, and RNA stability during transport and storage. A dried blood spot matrix for collecting high-quality RNA, called RNA Stabilizing Matrix (RSM), was evaluated against PAXgene® blood collection tubes. Methods Whole blood was collected from 25 individuals and subjected to 3 sample storage conditions: 18 hours at either room temperature (baseline arm) or 37°C, and 6 days at room temperature. RNA was extracted and assessed for integrity by Agilent Bioanalyzer, and gene expression was compared by RT-qPCR across 23 mRNAs comprising a clinical test for obstructive coronary artery disease. Results RSM produced RNA of relatively high integrity across the various tested conditions (mean RIN ± 95% CI: baseline arm, 6.92 ± 0.24; 37°C arm, 5.98 ± 0.48; 6-day arm, 6.72 ± 0.23). PAXgene samples showed comparable RNA integrity in both baseline and 37°C arms (8.42 ± 0.17; 7.92 ± 0.1 respectively) however significant degradation was observed in the 6-day arm (3.19 ± 1.32). Gene expression scores on RSM were highly correlated between the baseline and 37°C and 6-day study arms (median r = 0.96, 0.95 respectively), as was the correlation to PAXgene tubes (median r = 0.95, p < 0.001). Conclusion RNA obtained from RSM shows little degradation and comparable RT-qPCR performance to PAXgene RNA for the 23 genes analyzed. Further development of this technology may provide a convenient method for collecting, shipping, and storing RNA for gene expression assays. [ABSTRACT FROM AUTHOR]

Published
2014
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20. Discovery and validation of a novel subgroup and therapeutic targetin idiopathic multicentric Castleman disease

Author

Pierson, Sheila K., Shenoy, Sushila, Oromendia, Ana B., Gorzewski, Alexander, Pai, Ruth-Anne Langan, Nabel, Christopher Shield, Ruth, Jason R, Parente, Sophia A.T., Arenas, Daniel J., Guilfoyle, Mary, Reddy, Manjula, Weinblatt, Michael, Shadick, Nancy, Bower, Mark, Pria, Alessia Dalla, Masaki, Yasufumi, Katz, Laura, Mezey, Jason, Beineke, Philip, Lee, David, Tendler, Craig, Kambayashi, Taku, Fosså, Alexander, van Rhee, Frits, and Fajgenbaum, David C.

Abstract

Idiopathic multicentric Castleman disease (iMCD) is a poorly-understood hematologic disorder involving cytokine-induced polyclonal lymphoproliferation, systemic inflammation, and potentially-fatal multi-organ failure. Though the etiology of iMCD is unknown, interleukin-6 (IL-6) is an established disease driver in approximately one-third of patients. Anti-IL-6 therapy, siltuximab, is the only FDA-approved treatment. Few options exist for siltuximab non-responders, and no validated tests are available to predict likelihood of response. We procured and analyzed the largest-to-date cohort of iMCD samples, which enabled classification of iMCD into disease categories, discoveries of siltuximab response biomarkers, and identification of therapeutic targets for siltuximab non-responders. Proteomic quantification of 1,178 analytes was performed on serum of 88 iMCD patients, 60 patients with clinico-pathologically overlapping diseases(human herpesvirus-8(HHV8)-associated MCD, N=20; Hodgkin lymphoma, N=20; rheumatoid arthritis, N=20), and 44 healthy controls. Unsupervised clustering revealediMCD patients have heterogeneous serum proteomes that did not cluster with clinico-pathologically overlapping diseases. Clustering of iMCD patients identified a novel subgroup with superior responseto siltuximab, which wasvalidated using a 7-analyte panel (apolipoprotein E, amphiregulin, serum amyloid P-component,inactivatedcomplement C3b, immunoglobulin E, IL-6, erythropoietin)in an independent cohort. Enrichment analyses and immunohistochemistry identified JAK-STAT3 signaling as a candidate therapeutic targetthatcould potentially be targetedwith JAK inhibitorsin siltuximab non-responders. Ourdiscoveries demonstrate the potentialfor accelerating discoveries for rare diseases through multi-stakeholder collaboration.

Published
2021
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21. Datopotamab-deruxtecan in early-stage breast cancer: the sequential multiple assignment randomized I-SPY2.2 phase 2 trial.

Author

Khoury K, Meisel JL, Yau C, Rugo HS, Nanda R, Davidian M, Tsiatis B, Chien AJ, Wallace AM, Arora M, Rozenblit M, Hershman DL, Zimmer A, Clark AS, Beckwith H, Elias AD, Stringer-Reasor E, Boughey JC, Nangia C, Vaklavas C, Omene C, Albain KS, Kalinsky KM, Isaacs C, Tseng J, Roussos Torres ET, Thomas B, Thomas A, Sanford A, Balassanian R, Ewing C, Yeung K, Sauder C, Sanft T, Pusztai L, Trivedi MS, Outhaythip A, Li W, Onishi N, Asare AL, Beineke P, Norwood P, Brown-Swigart L, Hirst GL, Matthews JB, Moore B, Fraser Symmans W, Price E, Beedle C, Perlmutter J, Pohlmann P, Shatsky RA, DeMichele A, Yee D, van 't Veer LJ, Hylton NM, and Esserman LJ

Abstract

Among the goals of patient-centric care are the advancement of effective personalized treatment, while minimizing toxicity. The phase 2 I-SPY2.2 trial uses a neoadjuvant sequential therapy approach in breast cancer to further these goals, testing promising new agents while optimizing individual outcomes. Here we tested datopotamab-deruxtecan (Dato-DXd) in the I-SPY2.2 trial for patients with high-risk stage 2/3 breast cancer. I-SPY2.2 uses a sequential multiple assignment randomization trial design that includes three sequential blocks of biologically targeted neoadjuvant treatment: the experimental agent(s) (block A), a taxane-based regimen tailored to the tumor subtype (block B) and doxorubicin-cyclophosphamide (block C). Patients are randomized into arms consisting of different investigational block A treatments. Algorithms based on magnetic resonance imaging and core biopsy guide treatment redirection after each block, including the option of early surgical resection in patients predicted to have a high likelihood of pathological complete response, the primary endpoint. There are two primary efficacy analyses: after block A and across all blocks for the six prespecified breast cancer subtypes (defined by clinical hormone receptor/human epidermal growth factor receptor 2 (HER2) status and/or the response-predictive subtypes). We report results of 103 patients treated with Dato-DXd. While Dato-DXd did not meet the prespecified threshold for success (graduation) after block A in any subtype, the treatment strategy across all blocks graduated in the hormone receptor-negative HER2 - Immune - DNA repair deficiency - subtype with an estimated pathological complete response rate of 41%. No new toxicities were observed, with stomatitis and ocular events occurring at low grades. Dato-DXd was particularly active in the hormone receptor-negative/HER2 - Immune - DNA repair deficiency - signature, warranting further investigation, and was safe in other subtypes in patients who followed the treatment strategy. ClinicalTrials.gov registration: NCT01042379 ., (© 2024. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published
2024
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22. Datopotamab-deruxtecan plus durvalumab in early-stage breast cancer: the sequential multiple assignment randomized I-SPY2.2 phase 2 trial.

Author

Shatsky RA, Trivedi MS, Yau C, Nanda R, Rugo HS, Davidian M, Tsiatis B, Wallace AM, Chien AJ, Stringer-Reasor E, Boughey JC, Omene C, Rozenblit M, Kalinsky K, Elias AD, Vaklavas C, Beckwith H, Williams N, Arora M, Nangia C, Roussos Torres ET, Thomas B, Albain KS, Clark AS, Falkson C, Hershman DL, Isaacs C, Thomas A, Tseng J, Sanford A, Yeung K, Boles S, Chen YY, Huppert L, Jahan N, Parker C, Giridhar K, Howard FM, Blackwood MM, Sanft T, Li W, Onishi N, Asare AL, Beineke P, Norwood P, Brown-Swigart L, Hirst GL, Matthews JB, Moore B, Symmans WF, Price E, Heditsian D, LeStage B, Perlmutter J, Pohlmann P, DeMichele A, Yee D, van 't Veer LJ, Hylton NM, and Esserman LJ

Abstract

Sequential adaptive trial designs can help accomplish the goals of personalized medicine, optimizing outcomes and avoiding unnecessary toxicity. Here we describe the results of incorporating a promising antibody-drug conjugate, datopotamab-deruxtecan (Dato-DXd) in combination with programmed cell death-ligand 1 inhibitor, durvalumab, as the first sequence of therapy in the I-SPY2.2 phase 2 neoadjuvant sequential multiple assignment randomization trial for high-risk stage 2/3 breast cancer. The trial includes three blocks of treatment, with initial randomization to different experimental agent(s) (block A), followed by a taxane-based regimen tailored to tumor subtype (block B), followed by doxorubicin-cyclophosphamide (block C). Subtype-specific algorithms based on magnetic resonance imaging volume change and core biopsy guide treatment redirection after each block, including the option of early surgical resection in patients predicted to have a high likelihood of pathologic complete response, which is the primary endpoint assessed when resection occurs. There are two primary efficacy analyses: after block A and across all blocks for six prespecified HER2-negative subtypes (defined by hormone receptor status and/or response-predictive subtypes). In total, 106 patients were treated with Dato-DXd/durvalumab in block A. In the immune-positive subtype, Dato-DXd/durvalumab exceeded the prespecified threshold for success (graduated) after block A; and across all blocks, pathologic complete response rates were equivalent to the rate expected for the standard of care (79%), but 54% achieved that result after Dato-DXd/durvalumab alone (block A) and 92% without doxorubicin-cyclophosphamide (after blocks A + B). The treatment strategy across all blocks graduated in the hormone-negative/immune-negative subtype. No new toxicities were observed. Stomatitis was the most common side effect in block A. No patients receiving block A treatment alone had adrenal insufficiency. Dato-DXd/durvalumab is a promising therapy combination that can eliminate standard chemotherapy in many patients, particularly the immune-positive subtype.ClinicalTrials.gov registration: NCT01042379 ., (© 2024. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published
2024
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23. Mitral annular size predicts Alfieri stitch tension in mitral edge-to-edge repair.

Author

Timek TA, Nielsen SL, Lai DT, Tibayan F, Liang D, Daughters GT, Beineke P, Hastie T, Ingels NB Jr, and Miller DC

Subjects
Animals, Cardiopulmonary Bypass, Cardiotonic Agents administration & dosage, Dobutamine administration & dosage, Heart Rate drug effects, Heart Rate physiology, Heart Ventricles physiopathology, Heart Ventricles surgery, Male, Models, Animal, Models, Cardiovascular, Predictive Value of Tests, Sheep, Statistics as Topic, Stroke Volume drug effects, Stroke Volume physiology, Systole drug effects, Systole physiology, Time Factors, Ventricular Pressure drug effects, Ventricular Pressure physiology, Heart Valve Prosthesis Implantation, Mitral Valve physiopathology, Mitral Valve surgery, Suture Techniques
Abstract

Background and Aim of the Study: Whilst increased 'Alfieri stitch' tension may reduce the durability of 'edge-to-edge' mitral repair, the factors affecting suture tension are unknown. In order to study hemodynamics and left ventricular (LV) and annular dynamics that determine suture tension, the central edge of the mitral leaflets was approximated with a miniature force transducer to measure leaflet tension (T) at the leaflet approximation point., Methods: Eight sheep were studied under open-chest conditions immediately after surgical placement of a force transducer and implantation of radiopaque markers on the left ventricle and mitral annulus (MA). Hemodynamic variables were altered by two caval occlusion steps (deltaV1 and deltaV2) and dobutamine infusion. Three-dimensional marker coordinates were obtained by simultaneous biplane videofluoroscopy to measure LV volume, MA area (MAA) and septal-lateral (SL) annular dimension throughout the cardiac cycle., Results: At baseline, peak Alfieri stitch tension (0.30 +/- 0.18 N) was observed 96 +/- 61 ms prior to end-diastole coincident with peak annular SL diameter (98 +/- 58 ms before end-diastole). Dobutamine infusion decreased suture tension (from 0.30 +/- 0.18 N to 0.20 +/- 0.12 N, p = 0.01), although peak systolic pressure increased significantly (138 +/- 19 versus 115 +/- 14 mmHg; p = 0.03). A regression model was fitted with the goal of interpreting the hemodynamic and geometric predictors of tension as their influence varied with time: Tt (N) = 0.1916 + 0.2115 x SL (cm) - 0.1996 x MAA/SL (cm2/cm) + ft x LVP (mmHg), where Tt is tension at any time during the cardiac cycle and ft is the time-varying coefficient of LVP., Conclusion: Tension on the leaflets in the edge-to-edge repair is determined primarily by MA SL size, and paradoxically is lower when the contractile state is enhanced. This indicates that annular and/or LV dilatation increase stitch tension and may adversely affect durability of the repair if concomitant ring annuloplasty is not performed.

Published
2004

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